• 제목/요약/키워드: virtual refractor

검색결과 2건 처리시간 0.019초

가상 굴절검사 교육에 대한 평가 (An Evaluation of the Virtual Refraction Education)

  • 유동식;손정식;추병선
    • 한국안광학회지
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    • 제13권2호
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    • pp.43-50
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    • 2008
  • 목적: 실제 굴절검사(PR, Practical Refraction)를 위한 교육용 시뮬레이터인 가상 굴절검사(VR, Virtual Refractor) 의 효과를 평가하는데 있다. 방법: 안경광학과 3학년에 재학 중인 24명이 VR교육에 지원하였다. 학생 스스로 VR교육에 참가하여 연습을 하였고, 1개월 후 학생들은 가상 굴절검사에서 가상 피검자 3명과 실제 굴절검사에서 실제 피검자 1명에 대해 굴절검사를 실시하여 평가 결과를 제출하였고, 가상과 실제 굴절검사의 평가 결과를 비교하였다. 또한 5점 리커척도를 기준으로 한 자가 평가 설문을 자발적 참여도, 굴절검사에 대한 기여도, VR과 PR의 일치도 및 VR의 필요성과 같은 영역에 대하여 실시하였다. 결과: 가상 굴절검사와 실제 굴절검사의 평가에서 Spearman 상관계수는 0.71(p<0.01)로 뚜렷한 상관관계를 보였다. 설문에서 영역들의 평균은 3.67${\pm}$0.96로 VR 이용이 유익한 것으로 나타났고, 이들 영역 간에 0.91~0.68(p<0.01)의 높은 상관관계를 보였다. 결론: VR은 연습의 집중도를 높이고 실제 상황에 맞는 체계적 접근과 역할이 되도록 보완이 필요하지만, VR과 실제 굴절검사 사이에 높은 상관성을 보 였으며 VR은 실제 굴절검사에 도움이 되는 긍정적 평가를 보였다.

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Identification and Validation of Novel Biomarkers and Potential Targeted Drugs in Cholangiocarcinoma: Bioinformatics, Virtual Screening, and Biological Evaluation

  • Wang, Jiena;Zhu, Weiwei;Tu, Junxue;Zheng, Yihui
    • Journal of Microbiology and Biotechnology
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    • 제32권10호
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    • pp.1262-1274
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    • 2022
  • Cholangiocarcinoma (CCA) is a complex and refractor type of cancer with global prevalence. Several barriers remain in CCA diagnosis, treatment, and prognosis. Therefore, exploring more biomarkers and therapeutic drugs for CCA management is necessary. CCA gene expression data was downloaded from the TCGA and GEO databases. KEGG enrichment, GO analysis, and protein-protein interaction network were used for hub gene identification. miRNA were predicted using Targetscan and validated according to several GEO databases. The relative RNA and miRNA expression levels and prognostic information were obtained from the GEPIA. The candidate drug was screened using pharmacophore-based virtual screening and validated by molecular modeling and through several in vitro studies. 301 differentially expressed genes (DEGs) were screened out. Complement and coagulation cascades-related genes (including AHSG, F2, TTR, and KNG1), and cell cycle-related genes (including CDK1, CCNB1, and KIAA0101) were considered as the hub genes in CCA progression. AHSG, F2, TTR, and KNG1 were found to be significantly decreased and the eight predicted miRNA targeting AHSG, F2, and TTR were increased in CCA patients. CDK1, CCNB1, and KIAA0101 were found to be significantly abundant in CCA patients. In addition, Molport-003-703-800, which is a compound that is derived from pharmacophores-based virtual screening, could directly bind to CDK1 and exhibited anti-tumor activity in cholangiocarcinoma cells. AHSG, F2, TTR, and KNG1 could be novel biomarkers for CCA. Molport-003-703-800 targets CDK1 and work as potential cell cycle inhibitors, thereby having potential for consideration for new chemotherapeutics for CCA.